Author: Comert, Fatih; Heinrich, Frank; Chowdhury, Ananda; Schoeneck, Mason; Darling, Caitlin; Anderson, Kyle W.; Libardo, M. Daben J.; Angeles-Boza, Alfredo M.; Silin, Vitalii; Cotten, Myriam L.; Mihailescu, Mihaela
Title: Copper-binding anticancer peptides from the piscidin family: an expanded mechanism that encompasses physical and chemical bilayer disruption Cord-id: bk7zczdk Document date: 2021_6_16
ID: bk7zczdk
Snippet: In the search for novel broad-spectrum therapeutics to fight chronic infections, inflammation, and cancer, host defense peptides (HDPs) have garnered increasing interest. Characterizing their biologically-active conformations and minimum motifs for function represents a requisite step to developing them into efficacious and safe therapeutics. Here, we demonstrate that metallating HDPs with Cu(2+) is an effective chemical strategy to improve their cytotoxicity on cancer cells. Mechanistically, we
Document: In the search for novel broad-spectrum therapeutics to fight chronic infections, inflammation, and cancer, host defense peptides (HDPs) have garnered increasing interest. Characterizing their biologically-active conformations and minimum motifs for function represents a requisite step to developing them into efficacious and safe therapeutics. Here, we demonstrate that metallating HDPs with Cu(2+) is an effective chemical strategy to improve their cytotoxicity on cancer cells. Mechanistically, we find that prepared as Cu(2+)-complexes, the peptides not only physically but also chemically damage lipid membranes. Our testing ground features piscidins 1 and 3 (P1/3), two amphipathic, histidine-rich, membrane-interacting, and cell-penetrating HDPs that are α-helical bound to membranes. To investigate their membrane location, permeabilization effects, and lipid-oxidation capability, we employ neutron reflectometry, impedance spectroscopy, neutron diffraction, and UV spectroscopy. While P1-apo is more potent than P3-apo, metallation boosts their cytotoxicities by up to two- and seven-fold, respectively. Remarkably, P3-Cu(2+) is particularly effective at inserting in bilayers, causing water crevices in the hydrocarbon region and placing Cu(2+) near the double bonds of the acyl chains, as needed to oxidize them. This study points at a new paradigm where complexing HDPs with Cu(2+) to expand their mechanistic reach could be explored to design more potent peptide-based anticancer therapeutics.
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